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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >A novel IRQ ligand-modified nano-carrier targeted to a unique pathway of caveolar endocytic pathway
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A novel IRQ ligand-modified nano-carrier targeted to a unique pathway of caveolar endocytic pathway

机译:一种新型的IRQ配体修饰的纳米载体,靶向小窝内吞途径的独特途径

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摘要

In the present study, the cellular uptake and subsequent intracellular trafficking of liposomes was investigated, in which a novel peptide (IRQ), identified with in vivo phage display, was modified on the surface. Since the novel peptide IRQRRRR is rich in arginine, the cellular uptake mechanism was compared with octaarginine (R8)-modified liposomes, which are known to be taken up by cells via macropinocytosis. The uptake mechanism and intracellular trafficking of peptide-modified liposomes was determined by confocal laser scanning microscopy and flow cytometry analysis. Modification of the liposomal surface with the IRQ peptide (IRQ-Lip), induced internalization via a novel pathway-caveolar endocytosis-in parallel with clathrin-mediated endocytosis, Furthermore, the IRQ peptide stimulated escape from endocytic vesicles, leading to efficient gene silencing. When siRNA was condensed and encapsulated in an IRQ-modified multifunctional envelope-type nano-device (IRQ-MEND), transgene expression was reduced 52% with the fusogenic lipid, DOPE/CHEMS. This result shows that the novel IRQ can be utilized for cytoplasmic delivery of macromolecules. Moreover, the IRQ has the potential to be useful for delivery therapeutic agents to parenchymal cells via caveolar endocytosis, as this uptake pathway also plays an important role in transcytosis. (C) 2007 Elsevier B.V. All rights reserved.
机译:在本研究中,研究了脂质体的细胞摄取和随后的细胞内运输,其中在体内修饰了用体内噬菌体展示鉴定的新型肽(IRQ)。由于新型肽IRQRRRR富含精氨酸,因此将细胞摄取机制与八精氨酸(R8)修饰的脂质体进行了比较,已知脂质体是通过巨胞吞作用被细胞摄取的。通过共聚焦激光扫描显微镜和流式细胞仪分析确定了肽修饰的脂质体的摄取机制和细胞内运输。用IRQ肽(IRQ-Lip)修饰脂质体表面,通过新颖的途径-肺泡内吞作用-与网格蛋白介导的内吞作用同时诱导内在化。此外,IRQ肽刺激内吞小泡逃逸,从而导致有效的基因沉默。当将siRNA浓缩并封装在IRQ修饰的多功能包膜型纳米器件(IRQ-MEND)中时,融合脂质DOPE / CHEMS可将转基因表达降低52%。该结果表明新型IRQ可用于大分子的细胞质递送。此外,IRQ可能可用于通过小窝内吞作用将治疗剂递送至实质细胞,因为这种摄取途径在转胞作用中也起着重要作用。 (C)2007 Elsevier B.V.保留所有权利。

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